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羟基酪醇影响运动诱导的大鼠线粒体呼吸复合物向超复合物的组装。

Hydroxytyrosol influences exercise-induced mitochondrial respiratory complex assembly into supercomplexes in rats.

机构信息

Institute of Nutrition and Food Technology, Biomedical Research Centre, Department of Physiology, Faculty of Sport Sciences, University of Granada, Avda del conocimiento s/n. 18016 Armilla, Granada, Spain.

Institute of Biotechnology, Biomedical Research Centre, Department of Physiology, Faculty of Medicine, University of Granada, Avda del conocimiento s/n. 18016 Armilla, Granada, Spain.

出版信息

Free Radic Biol Med. 2019 Apr;134:304-310. doi: 10.1016/j.freeradbiomed.2019.01.027. Epub 2019 Jan 24.

Abstract

Hydroxytyrosol (HT) has been demonstrated to improve mitochondrial function, both in sedentary and in exercised animals. Herein, we assessed the effects of two different doses of HT on exercise-induced mitochondrial respiratory complex (C) assembly into supercomplexes (SCs) and the relation of the potential results to OPA1 levels and oxidative stress. Wistar rats were allocated into six groups: sedentary (SED), sedentary consuming 20 mg/kg/d of HT (SED-20), sedentary consuming 300 mg/kg/d of HT (SED-300); exercised (EXE), exercised consuming 20 mg/kg/d of HT (EXE-20) and exercised consuming 300 mg/kg/d of HT (EXE-300). Animals were exercised and/or supplemented for 10 weeks, and assembly of SCs, mitochondrial oxidative status and expression of OPA1 were quantified in the gastrocnemius muscle. Both EXE and EXE-20 animals exhibited increased assembly of CI into SCs, but this effect was absent in EXE-300 animals. Levels of CIII assembled into SCs were only increased in EXE-20 animals. Notably EXE-300 animals showed a decreased relative expression of s-OPA1 isoforms. Therefore, HT exerted dose-dependent effects on SC assembly in exercised animals. Although the mechanisms leading to SCs assembly in response to exercise and HT are unclear, it seems that a high HT dose can prevent SCs assembly during exercise by decreasing the expression of the s-OPA1 isoforms.

摘要

羟基酪醇(HT)已被证明可改善静止和运动动物的线粒体功能。在此,我们评估了两种不同剂量的 HT 对运动诱导的线粒体呼吸复合物(C)组装成超复合物(SCs)的影响,以及潜在结果与 OPA1 水平和氧化应激的关系。Wistar 大鼠被分为六组:安静(SED)、安静状态下摄入 20mg/kg/d HT(SED-20)、安静状态下摄入 300mg/kg/d HT(SED-300);运动(EXE)、运动状态下摄入 20mg/kg/d HT(EXE-20)和运动状态下摄入 300mg/kg/d HT(EXE-300)。动物接受 10 周的运动和/或补充治疗,然后在比目鱼肌中定量测定 SCs 的组装、线粒体氧化状态和 OPA1 的表达。EXE 和 EXE-20 动物的 CI 均增加了 SCs 的组装,但 EXE-300 动物则没有这种作用。只有 EXE-20 动物的 CIII 组装成 SCs 的水平增加。值得注意的是,EXE-300 动物的 s-OPA1 同工型相对表达减少。因此,HT 对运动动物的 SC 组装产生了剂量依赖性影响。尽管运动和 HT 引起 SC 组装的机制尚不清楚,但似乎高 HT 剂量可以通过降低 s-OPA1 同工型的表达来防止运动期间 SCs 的组装。

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